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Mapping the global evidence base of bundibugyo ebolavirus disease: a systematic scoping review of research gaps and preparedness priorities.

Created on 10 Jul 2026

Authors

Abigail Boatemaa, Baffour Osei, Gabriel Osei Forkuo

Published in

BMC infectious diseases. Jul 09, 2026. Epub Jul 09, 2026.

Abstract

Bundibugyo ebolavirus (BDBV) is a rare filovirus species with an estimated case fatality rate (CFR) ranging from 25% to 51%. The 2026 BDBV outbreak in the Democratic Republic of the Congo (DRC) was declared a Public Health Emergency of International Concern (PHEIC), highlighting the critical necessity of assessing global research preparedness for this pathogen.
To systematically map the global scientific evidence base on BDBV, characterize temporal and thematic publication trends, identify critical knowledge gaps, and formulate actionable priorities for public health response and clinical research.
Following PRISMA-ScR guidelines, we programmatically searched PubMed/MEDLINE, OpenAlex, and Semantic Scholar for literature published from 2007 through May 2026. From 4,379 screened records, 100 high-relevance studies were selected using a weighted composite relevance scoring system. To structure the evidence, we synthesized a novel conceptual model mapping BDBV research across three core pillars-epidemiological drivers, health system responses, and public health outcomes-connected by a policy feedback loop and conditioned by cross-cutting systemic moderators (conflict, weak infrastructure, global governance, and research gaps). Methodological quality was evaluated using the Risk of Bias 2.0 (RoB 2) framework.
Only 23% of the included studies specifically addressed BDBV, with the remainder focusing on broader ebolavirus topics dominated by Ebola virus (EBOV). Applying the conceptual model revealed pronounced asymmetries across the research domains: the literature remains heavily concentrated within upstream epidemiological drivers and clinical features. Conversely, critical health system response domains lack validated tools; no licensed vaccine, specific therapeutic agent, or point-of-care rapid diagnostic test validated for BDBV currently exists. While cross-reactive monoclonal antibodies show preclinical efficacy, clinical-grade validation remains absent, and longitudinal survivor outcomes are sparsely documented. Systemic moderators, particularly weak health infrastructure and conflict, continue to compound these gaps. Methodological risk of bias was moderate, driven by missing outcome data (42% of studies) and selective reporting (41%).
BDBV remains understudied relative to its epidemic potential. Sustained, internationally coordinated investments modeled on prior EBOV frameworks are required to transition from reactive to proactive research models.
Not applicable.

PMID:
42426656
Bibliographic data and abstract were imported from PubMed on 10 Jul 2026.

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